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A furosemide – isonicotinamide cocrystal: An investigation of properties and extensive structural disorder

Kerr, Hannah E.; Softley, Lorna K.; Kuthuru, Suresh; Nangia, Ashwini; Hodgkinson, Paul; Evans, Ivana Radosavljevic

A furosemide – isonicotinamide cocrystal: An investigation of properties and extensive structural disorder Thumbnail


Authors

Hannah E. Kerr

Lorna K. Softley

Suresh Kuthuru

Ashwini Nangia



Abstract

Furosemide is a loop diuretic drug marketed in solid form which suffers from low solubility and low permeability. The pharmaceutically relevant properties of a recently described furosemide-isonicotinamide 2:1 cocrystal (2FS-INA) were investigated and compared with those of other known furosemide cocrystals. The intrinsic dissolution rate of 2FS-INA was found to be very similar to that of commercial FS, while its equilibrium solubility was 5.6 times higher than that of pure FS. The extensive structural disorder in 2FS-INA observed by diffraction methods was also investigated by variable-temperature solid-state NMR in conjunction with first principles calculations. 15N NMR confirmed the absence of proton disorder in the short OH...N hydrogen bond. The disordered sulphonamide group was found to be dynamic by variable temperature 2H experiments, involving fast exchange of the sulphonamide NH2 protons combined with a rotation of the whole sulphonamide group about the C-S bond. The disorder of the furan rings of both the unique furosemide molecules was also found to be dynamic by 13C experiments, with roughly the same activation barrier for both rings.

Citation

Kerr, H. E., Softley, L. K., Kuthuru, S., Nangia, A., Hodgkinson, P., & Evans, I. R. (2015). A furosemide – isonicotinamide cocrystal: An investigation of properties and extensive structural disorder. CrystEngComm, 17(35), 6707-6715. https://doi.org/10.1039/c5ce01183c

Journal Article Type Article
Acceptance Date Jul 29, 2015
Publication Date Sep 21, 2015
Deposit Date Jul 31, 2015
Publicly Available Date Jan 10, 2016
Journal CrystEngComm
Publisher Royal Society of Chemistry
Peer Reviewed Peer Reviewed
Volume 17
Issue 35
Pages 6707-6715
DOI https://doi.org/10.1039/c5ce01183c

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